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Long term ablation of protein kinase A (PKA)-mediated cardiac troponin I phosphorylation leads to excitation-contraction uncoupling and diastolic dysfunction in a knock-in mouse model of hypertrophic cardiomyopathy.在肥厚型心肌病的基因敲入小鼠模型中,蛋白激酶A(PKA)介导的心肌肌钙蛋白I磷酸化的长期消融会导致兴奋-收缩解偶联和舒张功能障碍。
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2
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3
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Selective phosphorylation of PKA targets after β-adrenergic receptor stimulation impairs myofilament function in Mybpc3-targeted HCM mouse model.β-肾上腺素受体刺激后 PKA 靶标的选择性磷酸化可损害 Mybpc3 靶向 HCM 小鼠模型中的肌丝功能。
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Anim Cells Syst (Seoul). 2025 Jul 28;29(1):446-468. doi: 10.1080/19768354.2025.2533821. eCollection 2025.
2
Mechano-energetic uncoupling in hypertrophic cardiomyopathy: Pathophysiological mechanisms and therapeutic opportunities.肥厚型心肌病中的机械-能量解偶联:病理生理机制与治疗机遇
J Mol Cell Cardiol Plus. 2023 May 6;4:100036. doi: 10.1016/j.jmccpl.2023.100036. eCollection 2023 Jun.
3
The effect of long-term administration of green tea catechins on aging-related cardiac diastolic dysfunction and decline of troponin I.长期服用绿茶儿茶素对衰老相关心脏舒张功能障碍及肌钙蛋白I下降的影响。
Genes Dis. 2024 Apr 3;12(2):101284. doi: 10.1016/j.gendis.2024.101284. eCollection 2025 Mar.
4
The abnormalities of free fatty acid metabolism in patients with hypertrophic cardiomyopathy, a single-center retrospective observational study.肥厚型心肌病患者游离脂肪酸代谢异常:一项单中心回顾性观察研究。
BMC Cardiovasc Disord. 2024 Jun 20;24(1):312. doi: 10.1186/s12872-024-03925-9.
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Assessing Cardiac Contractility From Single Molecules to Whole Hearts.从单分子到全心脏评估心脏收缩力
JACC Basic Transl Sci. 2023 Oct 11;9(3):414-439. doi: 10.1016/j.jacbts.2023.07.013. eCollection 2024 Mar.
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本文引用的文献

1
Perturbed length-dependent activation in human hypertrophic cardiomyopathy with missense sarcomeric gene mutations.肌节基因突变致肥厚型心肌病中受干扰的长度依赖性激活。
Circ Res. 2013 May 24;112(11):1491-505. doi: 10.1161/CIRCRESAHA.111.300436. Epub 2013 Mar 18.
2
Hydralazine and organic nitrates restore impaired excitation-contraction coupling by reducing calcium leak associated with nitroso-redox imbalance.肼屈嗪和有机硝酸盐通过减少与亚硝基氧化还原失衡相关的钙漏来恢复受损的兴奋-收缩偶联。
J Biol Chem. 2013 Mar 1;288(9):6522-33. doi: 10.1074/jbc.M112.412130. Epub 2013 Jan 14.
3
Late sodium current inhibition reverses electromechanical dysfunction in human hypertrophic cardiomyopathy.晚期钠电流抑制可逆转人类肥厚型心肌病的机电功能障碍。
Circulation. 2013 Feb 5;127(5):575-84. doi: 10.1161/CIRCULATIONAHA.112.134932. Epub 2012 Dec 27.
4
Shortening baroreflex delay in hypertrophic cardiomyopathy patients -- an unknown effect of β-blockers.缩短肥厚型心肌病患者的压力感受反射时滞——β受体阻滞剂的未知作用。
Br J Clin Pharmacol. 2013 Jun;75(6):1516-24. doi: 10.1111/bcp.12027.
5
Myofibrillar Ca(2+) sensitivity is uncoupled from troponin I phosphorylation in hypertrophic obstructive cardiomyopathy due to abnormal troponin T.由于肌钙蛋白 T 的异常,肥厚型梗阻性心肌病中的肌原纤维 Ca(2+) 敏感性与肌钙蛋白 I 磷酸化脱耦联。
Cardiovasc Res. 2013 Mar 1;97(3):500-8. doi: 10.1093/cvr/cvs322. Epub 2012 Oct 24.
6
Multiple reaction monitoring to identify site-specific troponin I phosphorylated residues in the failing human heart.采用多重反应监测法鉴定衰竭人心肌肌钙蛋白 I 特定位点磷酸化残基。
Circulation. 2012 Oct 9;126(15):1828-37. doi: 10.1161/CIRCULATIONAHA.112.096388. Epub 2012 Sep 12.
7
Hypertrophic cardiomyopathy.肥厚型心肌病。
Lancet. 2013 Jan 19;381(9862):242-55. doi: 10.1016/S0140-6736(12)60397-3. Epub 2012 Aug 6.
8
Myosin binding protein-C phosphorylation is the principal mediator of protein kinase A effects on thick filament structure in myocardium.肌球蛋白结合蛋白-C 磷酸化是蛋白激酶 A 对心肌粗丝结构产生影响的主要介质。
J Mol Cell Cardiol. 2012 Nov;53(5):609-16. doi: 10.1016/j.yjmcc.2012.07.012. Epub 2012 Jul 28.
9
Diastolic dysfunction and thin filament dysregulation resulting from excitation-contraction uncoupling in a mouse model of restrictive cardiomyopathy.舒张功能障碍和薄丝肌调节异常导致的兴奋-收缩脱偶联在限制型心肌病的小鼠模型中。
J Mol Cell Cardiol. 2012 Sep;53(3):446-57. doi: 10.1016/j.yjmcc.2012.05.018. Epub 2012 Jun 6.
10
Contractile dysfunction irrespective of the mutant protein in human hypertrophic cardiomyopathy with normal systolic function.收缩功能障碍与人类肥厚型心肌病的收缩功能正常无关,无论突变蛋白如何。
Circ Heart Fail. 2012 Jan;5(1):36-46. doi: 10.1161/CIRCHEARTFAILURE.111.963702. Epub 2011 Dec 16.

在肥厚型心肌病的基因敲入小鼠模型中,蛋白激酶A(PKA)介导的心肌肌钙蛋白I磷酸化的长期消融会导致兴奋-收缩解偶联和舒张功能障碍。

Long term ablation of protein kinase A (PKA)-mediated cardiac troponin I phosphorylation leads to excitation-contraction uncoupling and diastolic dysfunction in a knock-in mouse model of hypertrophic cardiomyopathy.

作者信息

Dweck David, Sanchez-Gonzalez Marcos A, Chang Audrey N, Dulce Raul A, Badger Crystal-Dawn, Koutnik Andrew P, Ruiz Edda L, Griffin Brittany, Liang Jingsheng, Kabbaj Mohamed, Fincham Frank D, Hare Joshua M, Overton J Michael, Pinto Jose R

机构信息

Department of Biomedical Sciences, Florida State University College of Medicine, Tallahassee, Florida 32306-4300.

Department of Biomedical Sciences, Florida State University College of Medicine, Tallahassee, Florida 32306-4300,; Family Institute, Florida State University, Tallahassee, Florida 32306.

出版信息

J Biol Chem. 2014 Aug 15;289(33):23097-23111. doi: 10.1074/jbc.M114.561472. Epub 2014 Jun 27.

DOI:10.1074/jbc.M114.561472
PMID:24973218
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4132808/
Abstract

The cardiac troponin I (cTnI) R21C (cTnI-R21C) mutation has been linked to hypertrophic cardiomyopathy and renders cTnI incapable of phosphorylation by PKA in vivo. Echocardiographic imaging of homozygous knock-in mice expressing the cTnI-R21C mutation shows that they develop hypertrophy after 12 months of age and have abnormal diastolic function that is characterized by longer filling times and impaired relaxation. Electrocardiographic analyses show that older R21C mice have elevated heart rates and reduced cardiovagal tone. Cardiac myocytes isolated from older R21C mice demonstrate that in the presence of isoproterenol, significant delays in Ca(2+) decay and sarcomere relaxation occur that are not present at 6 months of age. Although isoproterenol and stepwise increases in stimulation frequency accelerate Ca(2+)-transient and sarcomere shortening kinetics in R21C myocytes from older mice, they are unable to attain the corresponding WT values. When R21C myocytes from older mice are treated with isoproterenol, evidence of excitation-contraction uncoupling is indicated by an elevation in diastolic calcium that is frequency-dissociated and not coupled to shorter diastolic sarcomere lengths. Myocytes from older mice have smaller Ca(2+) transient amplitudes (2.3-fold) that are associated with reductions (2.9-fold) in sarcoplasmic reticulum Ca(2+) content. This abnormal Ca(2+) handling within the cell may be attributed to a reduction (2.4-fold) in calsequestrin expression in conjunction with an up-regulation (1.5-fold) of Na(+)-Ca(2+) exchanger. Incubation of permeabilized cardiac fibers from R21C mice with PKA confirmed that the mutation prevents facilitation of mechanical relaxation. Altogether, these results indicate that the inability to enhance myofilament relaxation through cTnI phosphorylation predisposes the heart to abnormal diastolic function, reduced accessibility of cardiac reserves, dysautonomia, and hypertrophy.

摘要

心肌肌钙蛋白I(cTnI)的R21C(cTnI-R21C)突变与肥厚型心肌病有关,并且使cTnI在体内无法被蛋白激酶A磷酸化。对表达cTnI-R21C突变的纯合敲入小鼠进行超声心动图成像显示,它们在12个月龄后出现心肌肥厚,并且舒张功能异常,其特征为舒张期充盈时间延长和舒张功能受损。心电图分析表明,年龄较大的R21C小鼠心率升高且心迷走神经张力降低。从年龄较大的R21C小鼠分离出的心肌细胞表明,在存在异丙肾上腺素的情况下,Ca(2+)衰减和肌节舒张会出现显著延迟,而在6个月龄时不存在这种情况。尽管异丙肾上腺素和刺激频率的逐步增加会加速老年小鼠R21C心肌细胞中Ca(2+)瞬变和肌节缩短动力学,但它们无法达到相应的野生型值。当用异丙肾上腺素处理老年小鼠的R21C心肌细胞时,舒张期钙升高表明存在兴奋-收缩解偶联,这种升高与频率解离相关,且与较短的舒张期肌节长度无关。老年小鼠的心肌细胞具有较小的Ca(2+)瞬变幅度(2.3倍),这与肌浆网Ca(2+)含量的降低(2.9倍)有关。细胞内这种异常Ca(2+)处理可能归因于肌集钙蛋白表达降低(2.4倍)以及钠-钙交换体上调(1.5倍)。用蛋白激酶A孵育R21C小鼠的透化心肌纤维证实,该突变阻止了机械舒张的促进作用。总之,这些结果表明,无法通过cTnI磷酸化增强肌丝舒张使心脏易出现舒张功能异常、心脏储备可及性降低、自主神经功能障碍和心肌肥厚。